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A Spontaneous Ring-Opening Reaction Leads to a Repair-Resistant Thymine Oxidation Product in Genomic DNA.

Accepted version
Peer-reviewed

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Abstract

The alphabet of modified DNA bases goes beyond the conventional four letters, with biological roles being found for many such modifications. Herein, we describe the observation of a modified thymine base that arises from spontaneous N1 -C2 ring opening of the oxidation product 5-formyl uracil, after N3 deprotonation. We first observed this phenomenon in silico through ab initio calculations, followed by in vitro experiments to verify its formation at a mononucleoside level and in a synthetic DNA oligonucleotide context. We show that the new base modification (Trex , thymine ring expunged) can form under physiological conditions, and is resistant to the action of common repair machineries. Furthermore, we found cases of the natural existence of Trex while screening a number of human cell types and mESC (E14), thus suggesting potential biological relevance of this modification.

Description

Keywords

base modification, nucleic acids, oxidative damage, repair resistance, ring opening, thymine, Cell Line, Tumor, DNA, HeLa Cells, Humans, Molecular Structure, Oxidation-Reduction, Thymine

Journal Title

Chembiochem

Conference Name

Journal ISSN

1439-4227
1439-7633

Volume Title

21

Publisher

Wiley

Rights

All rights reserved
Sponsorship
Cancer Research UK (18618)
Wellcome Trust (209441/Z/17/Z)
Cancer Research UK (CB4330)
The University of Cambridge, Vice Chancellor’s Award (Cambridge Trust) and the Dudding & Stachulski Scholarship